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首页> 外文期刊>International immunopharmacology >Administration of adenovirus encoding anti-CD20 antibody gene induces B-cell deletion and alleviates lupus in the BWF1 mouse model.
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Administration of adenovirus encoding anti-CD20 antibody gene induces B-cell deletion and alleviates lupus in the BWF1 mouse model.

机译:在BWF1小鼠模型中,施用编码抗CD20抗体基因的腺病毒可诱导B细胞缺失并减轻狼疮。

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Increasing evidence demonstrates that pathological B cells play an essential role in the triggering and development of human systemic lupus erythematosus (SLE). A rational strategy for treating SLE might be to delete B cells thereby suppressing autoimmunity. Commercial monoclonal anti-CD20 antibody is widely used for treatment of B cell-related autoimmune disorders. However its long term use is limited by several factors including short half-life, high cost, and possible side effects of antibody protein therapy. Therefore, we constructed a recombinant adenovirus encoding the murine anti-CD20 antibody gene, and used it to immunize lupus-prone (BWF1) mice. Our data demonstrated that administration of adenovirus encoding the murine anti-CD20 antibody gene generated murine anti-CD20 antibody, which resulted in elimination of B cells in BWF1 mice. In addition, the anti-CD20 reduced serum anti-dsDNA antibody levels, impeded the development of proteinuria and improved the survival of BWF1 mice. These findings suggested that the adenovirus encoding murine anti-CD20 antibody gene might provide an alternative strategy for B cell-mediated diseases.
机译:越来越多的证据表明,病理性B细胞在人类系统性红斑狼疮(SLE)的触发和发育中起着至关重要的作用。治疗SLE的合理策略可能是删除B细胞,从而抑制自身免疫。商业单克隆抗CD20抗体被广泛用于治疗B细胞相关的自身免疫性疾病。然而,其长期使用受到几个因素的限制,包括半衰期短,成本高以及抗体蛋白治疗可能产生的副作用。因此,我们构建了编码鼠抗CD20抗体基因的重组腺病毒,并将其用于免疫易患狼疮(BWF1)的小鼠。我们的数据表明,编码鼠抗CD20抗体基因的腺病毒的产生产生了鼠抗CD20抗体,从而消除了BWF1小鼠的B细胞。此外,抗CD20降低了血清抗dsDNA抗体水平,阻碍了蛋白尿的发展并改善了BWF1小鼠的生存。这些发现表明,编码鼠抗CD20抗体基因的腺病毒可能为B细胞介导的疾病提供替代策略。

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